NADPH oxidase 2 plays a role in experimental corneal neovascularization

Chan, Elsa C.; Wijngaarden, Peter van; Chan, Elsie; Ngo, Darleen C.; Wang, Jiang-Hui; Peshavariya, Hitesh; Dusting, Gregory J.; Liu, Guei‐Sheung

doi:10.1042/cs20150103

Cited by 19 publications

(16 citation statements)

References 46 publications

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“…We confirmed that NOX2 is also necessary for the proangiogenic effect of dRP in vivo . This is in line with two recent studies showing a role for this member of the NOX family in the stimulation of angiogenesis in vivo , although it should be emphasized that these reports, in contrast to the present study, did not provide clarity on the underlying molecular mechanisms ( 10 , 70 ).…”

Section: Discussionsupporting

confidence: 87%

Direct Activation of NADPH Oxidase 2 by 2-Deoxyribose-1-Phosphate Triggers Nuclear Factor Kappa B-Dependent Angiogenesis

Vara

Watt

Fortunato

et al. 2018

Antioxidants & Redox Signaling

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Aims: Deoxyribose-1-phosphate (dRP) is a proangiogenic paracrine stimulus released by cancer cells, platelets, and macrophages and acting on endothelial cells. The objective of this study was to clarify how dRP stimulates angiogenic responses in human endothelial cells.Results: Live cell imaging, electron paramagnetic resonance, pull-down of dRP-interacting proteins, followed by immunoblotting, gene silencing of different NADPH oxidases (NOXs), and their regulatory cosubunits by small interfering RNA (siRNA) transfection, and experiments with inhibitors of the sugar transporter glucose transporter 1 (GLUT1) were utilized to demonstrate that dRP acts intracellularly by directly activating the endothelial NOX2 complex, but not NOX4. Increased reactive oxygen species generation in response to NOX2 activity leads to redox-dependent activation of the transcription factor nuclear factor kappa B (NF-κB), which, in turn, induces vascular endothelial growth factor receptor 2 (VEGFR2) upregulation. Using endothelial tube formation assays, gene silencing by siRNA, and antibody-based receptor inhibition, we demonstrate that the activation of NF-κB and VEGFR2 is necessary for the angiogenic responses elicited by dRP. The upregulation of VEGFR2 and NOX2-dependent stimulation of angiogenesis by dRP were confirmed in excisional wound and Matrigel plug vascularization assays in vivo using NOX2−/− mice.Innovation: For the first time, we demonstrate that dRP acts intracellularly and stimulates superoxide anion generation by direct binding and activation of the NOX2 enzymatic complex.Conclusions: This study describes a novel molecular mechanism underlying the proangiogenic activity of dRP, which involves the sequential activation of NOX2 and NF-κB and upregulation of VEGFR2. Antioxid. Redox Signal. 28, 110–130.

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Section: Discussionsupporting

confidence: 87%

Direct Activation of NADPH Oxidase 2 by 2-Deoxyribose-1-Phosphate Triggers Nuclear Factor Kappa B-Dependent Angiogenesis

Vara

Watt

Fortunato

et al. 2018

Antioxidants & Redox Signaling

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“…It is worth noting that the nitrate injury is associated with an induction of the proangiogenic VEGF-A but not profibrotic factor TGFβ1. 13 In contrast, NaOH injury stimulates the expression of both VEGF and TGFβ1 in the burnt corneas, consistent with recent findings by Gu et al 28 In this regard, both Nox2 and Nox4 appear to regulate the initial inflammation and neovascular responses in the corneas up to day 7 following chemical insults. The induction of TGFβ1 is ablated in burnt corneas from Nox4 KO mice, which actually show a lower degree of opacity and collagen accumulation in the burnt corneas when compared to the WT.…”

Section: Discussionsupporting

confidence: 85%

“…Interestingly, the details of these mechanisms of response to injury vary a little between different models of corneal injury. Chan et al 13 used acidic silver nitrate to inflict an injury to the corneal surface, and this results in an upregulation of Nox2 mRNA and a downregulation of the Nox4 gene over 7 days. In that study, Nox2 upregulation was found to be associated with inflammation and neovascularization in the burnt corneas.…”

Section: Discussionmentioning

confidence: 99%

“… 6 – 9 We and others have also shown key roles for Nox isoforms in retinal angiogenesis and neovascularization 10 – 12 and similar roles for NADPH oxidase 2 (Nox2) in wound healing and neovascularization following chemical burns in the cornea. 13 In this study, we sought to clarify the role of the Nox4 isoform in neovascularization and wound healing after an alkali burn injury, using Nox4 knockout mice. 14 …”

mentioning

confidence: 99%

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Wound Healing After Alkali Burn Injury of the Cornea Involves Nox4-Type NADPH Oxidase

Hakami

Dusting

Chan

et al. 2020

Invest. Ophthalmol. Vis. Sci.

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Purpose Corneal injury that occurs after burning with alkali initiates wound-healing processes, including inflammation, neovascularization, and fibrosis. Excessive reactions to injury can reduce corneal transparency and thereby compromise vision. The NADPH oxidase (Nox) enzyme complex is known to be involved in cell signaling for wound-healing angiogenesis, but its role in corneal neovascularization has been little studied. Methods The center corneas of wild-type and Nox4 knockout (KO) mice were injured with 3 µL 1 M NaOH, while the contralateral corneas remained untouched. On day 7, mRNA expression levels of NADPH oxidase isoforms, the proangiogenic factors VEGF-A and TGFβ1, and proinflammatory genes ICAM-1 and VCAM-1 were determined. Corneal neovascularization and fibrosis were visualized using PECAM-1 antibody and picrosirius red staining, respectively, on the same day. Results Expressions of both Nox2 and Nox4 gene isoforms as well as the above genes were markedly increased in the injured corneas at 7 days. Injured corneas showed neovascularization and fibrosis as well as an increase in clinical opacity score. All responses stimulated by alkali burn were abrogated in Nox4 KO mice. Conclusions Nox4 could be a new target to treat pathologic corneal wound-healing responses and such targeting might prevent blindness caused by burn injuries.

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“…Next, topical administration of 0.5% Alcaine for local anesthesia was performed, followed by pressing the tip of an applicator containing silver nitrate/potassium (Grafco) to the center of the cornea steadily for 8 seconds. 22 The excess of nitrate was eliminated by washing with 5 mL of saline solution. A burned cornea causing opacity on the eye was observed.…”

Section: Huvec-migration Assaymentioning

confidence: 99%

Preparation of arginine–glycine–aspartic acid-modified biopolymeric nanoparticles containing epigalloccatechin-3-gallate for targeting vascular endothelial cells to inhibit corneal neovascularization

Chang

Wang

Miyagawa

et al. 2016

IJN

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NADPH oxidase 2 plays a role in experimental corneal neovascularization

Cited by 19 publications

References 46 publications

Direct Activation of NADPH Oxidase 2 by 2-Deoxyribose-1-Phosphate Triggers Nuclear Factor Kappa B-Dependent Angiogenesis

Direct Activation of NADPH Oxidase 2 by 2-Deoxyribose-1-Phosphate Triggers Nuclear Factor Kappa B-Dependent Angiogenesis

Wound Healing After Alkali Burn Injury of the Cornea Involves Nox4-Type NADPH Oxidase

Preparation of arginine–glycine–aspartic acid-modified biopolymeric nanoparticles containing epigalloccatechin-3-gallate for targeting vascular endothelial cells to inhibit corneal neovascularization

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NADPH oxidase 2 plays a role in experimental corneal neovascularization

Cited by 19 publications

References 46 publications

Direct Activation of NADPH Oxidase 2 by 2-Deoxyribose-1-Phosphate Triggers Nuclear Factor Kappa B-Dependent Angiogenesis

Direct Activation of NADPH Oxidase 2 by 2-Deoxyribose-1-Phosphate Triggers Nuclear Factor Kappa B-Dependent Angiogenesis

Wound Healing After Alkali Burn Injury of the Cornea Involves Nox4-Type NADPH Oxidase

Preparation of arginine&ndash;glycine&ndash;aspartic acid-modified biopolymeric nanoparticles containing epigalloccatechin-3-gallate for targeting vascular endothelial cells to inhibit corneal neovascularization

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Preparation of arginine–glycine–aspartic acid-modified biopolymeric nanoparticles containing epigalloccatechin-3-gallate for targeting vascular endothelial cells to inhibit corneal neovascularization